Distinct Clinical Patterns and Immune Infiltrates Are Observed at Time of Progression on Targeted Therapy Versus Immune Checkpoint Blockade for Melanoma

Overview

Journal Oncoimmunology

Specialty Allergy & Immunology

Date 2016 May 4

PMID 27141370

Citations 36

Authors

Zachary A Cooper

Alexandre Reuben

Christine N Spencer

Peter A Prieto

Jacob L Austin-Breneman

Hong Jiang

Cara Haymaker

Vancheswaran Gopalakrishnan

Michael T Tetzlaff

Dennie T Frederick

Ryan J Sullivan

Rodabe N Amaria

Sapna P Patel

Patrick Hwu

Scott E Woodman

Isabella C Glitza

Adi Diab

Luis M Vence

Jaime Rodriguez-Canales

Edwin R Parra

Ignacio I Wistuba

Lisa M Coussens

Arlene H Sharpe

Keith T Flaherty

Jeffrey E Gershenwald

Lynda Chin

Michael A Davies

Karen Clise-Dwyer

James P Allison

Padmanee Sharma

Jennifer A Wargo

Affiliations

Soon will be listed here.

Abstract

We have made major advances in the treatment of melanoma through the use of targeted therapy and immune checkpoint blockade; however, clinicians are posed with therapeutic dilemmas regarding timing and sequence of therapy. There is a growing appreciation of the impact of antitumor immune responses to these therapies, and we performed studies to test the hypothesis that clinical patterns and immune infiltrates differ at progression on these treatments. We observed rapid clinical progression kinetics in patients on targeted therapy compared to immune checkpoint blockade. To gain insight into possible immune mechanisms behind these differences, we performed deep immune profiling in tumors of patients on therapy. We demonstrated low CD8 T-cell infiltrate on targeted therapy and high CD8 T-cell infiltrate on immune checkpoint blockade at clinical progression. These data have important implications, and suggest that antitumor immune responses should be assessed when considering therapeutic options for patients with melanoma.

Citing Articles

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